Lichen Early Treatment for Alopecia Areata Prevention ... · 1 What are the causes of alopecia...

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Lichen

planopilaris

Pseudopelade

BrocqCCLE

CCLE

Folliculitis

decalvans

Early Treatment for Alopecia

Areata Prevention (ETAAP)

Matthew Harries

Consultant Dermatologist & Honorary Senior Lecturer The University of Manchester

Salford Royal NHS Foundation TrustManchester

UK

EBM Hair Update 15th May 2019

Good to be Back [1]!

Good to be Back [2]!

! hairs

Black dots

Yellow dots

“Leaving alopecia areata untreated is a legitimate option for many patients”

“Spontaneous remission occurs in up to 80%of patients with limited patchy hair loss of short

duration (< 1 year).”

“If there is no hair regrowth and there is less than 50% hair loss, discuss the option of watchful waiting with no

current treatment needed”

• Contacted 16-23 years later

• Significant tendency for AA to worsen with time

• 19% with mild disease (<50% area) had AT / AU at follow-up

• 93% with AU still had extensive disease (AT / AU) at follow-up

• 3% with extensive disease (AT / AU) were disease free at follow-up

Poor Prognosis in AA

• Extensive disease

• Long disease duration

• Onset before puberty

• Atopy

• Associated autoimmune disease

• Nail disease

• Positive FH

522 AA pts with >30 % AT/AU

SRFT Hair Clinic (2013 – present)

[n=1883]

AA

Scarring

TE

FPHL/MPHL

Traction

ChemoRx

Genetic

Other

Impact on the NHS

• Multiple unsuccessful treatments• Clinic visits

• Treatment / monitoring costs

• Estimated cost for DPC + wig treatment in Glasgow = £1500 per patient / year

(Phillips R, Holmes S. WCHR Abstract 2019)

STANDARD TREATMENT PATHWAY

Topical / Intralesional Steroids

DPC Dithranol

Systemic Steroids

PUVA Ciclosporin MTX

(JAKi / Others)

Significant Psychological Impact

Significant Psychological Impact

Rank Uncertainty

1 What are the causes of alopecia areata? For example, medications, medical problems, lifestyle,vaccinations

2 Are immunosuppressant therapies (e.g. methotrexate; mycophenolate mofitil) better than placebo in the treatment of alopecia areata?

3 In alopecia areata, are biological therapies (including janus kinase (JAK) inhibitors and anti-cytokine therapies) more effective than placebo in causing hair regrowth?

4 Are psychological interventions helpful in alopecia areata?

5 Can progression of alopecia areata be prevented by early diagnosis and treatment?

6 Do certain foods, vitamins or nutritional supplements improve hair regrowth in alopecia areata?

7 What can be learnt about alopecia areata from other autoimmune conditions?

8 In whom does alopecia areata hair loss progress and why?

9 Do any treatments have a long-term therapeutic benefit in alopecia areata?

10 How effective are alternative therapies in alopecia areata?

Alopecia Areata Priority Setting Partnership (PSP)

(MacBeth et al. Br J Dermatol 2017)

Rank Uncertainty

1 What are the causes of alopecia areata? For example, medications, medical problems, lifestyle,vaccinations

2 Are immunosuppressant therapies (e.g. methotrexate; mycophenolate mofitil) better than placebo in the treatment of alopecia areata?

3 In alopecia areata, are biological therapies (including janus kinase (JAK) inhibitors and anti-cytokine therapies) more effective than placebo in causing hair regrowth?

4 Are psychological interventions helpful in alopecia areata?

5 Can progression of alopecia areata be prevented by early diagnosis and treatment?

6 Do certain foods, vitamins or nutritional supplements improve hair regrowth in alopecia areata?

7 What can be learnt about alopecia areata from other autoimmune conditions?

8 In whom does alopecia areata hair loss progress and why?

9 Do any treatments have a long-term therapeutic benefit in alopecia areata?

10 How effective are alternative therapies in alopecia areata?

Alopecia Areata Priority Setting Partnership (PSP)

(MacBeth et al. Br J Dermatol 2017)

Lessons from other Immune-Mediated Inflammatory Disorders (IMID)

Aggressive early intervention in RA, Crohn’s disease & MS:

Reduce tissue damage and longer-term complications

Induces disease-free remission

(Girolomoni et al. J Dermatol Treat 2015)

Is there any Evidence that Early Treatment effects Prognosis in AA?

“There is no good trial evidence that any treatment provide long-term benefit to patients with alopecia areata, alopecia

totalis and alopecia universalis.”

2008

Clinical Observation: Better Outcomes with Early Treatment?

• 68 Pt with chronic AA treated with systemic therapy and followed for 2-7 years

• Rates of AT/AU = 17.6% [Expected rate 45% based on Ikeda data]

• Rationale to treat chronic AA to prevent AT/AU

(Cranwell et al. Aus J Dermatol 2018)

• Shorter duration between disease onset and treatment commencement

• “good” prognosis in children <10yrs old with “early onset” AA

(Suh et al. Ann Dermatol 2014)

• Treatment with pulsed systemic corticosteroids for extensive AA

• more effective, and less likely to relapse, when started within 1 year of disease onset compared with treatments commenced later on

(Yang et al. Ann Dermatol 2013)

Clinical Observation: AA Recurring at Previously Affected Sites

Original patch

12 Months

Relapse at same site

If previously affected skin is more susceptible to future attack = Argues for aggressive early treatment to prevent more

extensive scalp involvement

(Li & Sinclair. Aus J Dermatol 2016)

Is there Any Biological Rationale for Early Treatment?As there is no tissue damage in AA

Alopecia Areata – Bulb IP Collapse

NormalAA

(From Divito and Kupper. Nat Med 2014)

Positive feedback loop in AA

As has been proposed in Psoriasis, it is conceivable that stimulation of a small region of AA-predisposed skin results in an immune reaction that leads to the

development of lesions at local and distant body sites

(Girolomoni et al. J Dermatol Treat 2015)

• Disease recrudesce in susceptible tissue• Ongoing immune dysfunction / Sub-clinical inflammation?

• Incomplete IP restoration?

• “Molecular scar” (Girolomoni et al. J Dermatol Treat 2015)

Testing the HypothesisEarly treatment can prevent disease progression in AA

• Target those most likely to benefit from early treatment

• Improve Q of L & Reduce social stigmatisation

• Modify the disease course

Achieving prolonged medication-free remission

• Cost-effective management strategies

A Successful Early Treatment Strategy in AA would:

“Classic”

Single intervention vs. placebo given early in disease course

“Pragmatic”

Early intervention (of whatever type) vs. deferred treatment

Early Treatment for

Alopecia Areata Prevention

(ETAAP)

Possible Trial Design....

Early Treatment for

Alopecia Areata Prevention

(ETAAP)

Feasibility work...

• Target population and barriers to recruitmentEarly case identification

Acceptability of interventions

• Preferred outcome measures

• Power calculation

• Potential economic impact

Early Treatment for

Alopecia Areata Prevention

(ETAAP)

Feasibility work...

• Target population and barriers to recruitmentEarly case identification

Acceptability of interventions

• Preferred outcome measures

• Power calculation

• Potential economic impact

...eventually Leading to a Clinical Trial

Engagement with Primary CareSurveysFocus group workStatistics Advice

• Building the Team• Dermatologists / Patient / GPwSI / (Qualitative researcher) / Statistician

• Seeking advice• University of Manchester Primary Care Academic Unit • NIHR Research Design Service (RDS)• UK-DCTN

• Secured Funding• Alopecia UK

• Ethics• NIHR Portfolio adoption

• PUBLISH RESULTS

ETAAP: Progress

matthew.harries@srft.nhs.uk

The Dermatology CentreSalford Royal NHS Foundation Trust

Tel. 0161 2068015

Abby MacBeth, Andrew Messenger, Susan Holmes, Leila Asfour, Calvin Heald